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来自人类供体的血清对与恶性疟原虫环子孢子蛋白N端和C端非重复区域相对应的合成104肽和102肽的识别。

Recognition of synthetic 104-mer and 102-mer peptides corresponding to N- and C-terminal nonrepeat regions of the Plasmodium falciparum circumsporozoite protein by sera from human donors.

作者信息

Lopez J A, Roggero M A, Duombo O, Gonzalez J M, Tolle R, Koita O, Arevalo-Herrera M, Herrera S, Corradin G

机构信息

Institut de Biochimie, Universite de Lausanne, Epalinges, Switzerland.

出版信息

Am J Trop Med Hyg. 1996 Oct;55(4):424-9. doi: 10.4269/ajtmh.1996.55.424.

Abstract

In the present work, we analyze the recognition of synthetic polypeptides encompassing the aminoterminal (amino acids 22-125) and the carboxy terminal (289-390) regions of the circumsporozoite (CS) protein of Plasmodium falciparum by sera from donors living in endemic area of South America and Africa. Two populations were studied: one on the Colombian Pacific coast, with low endemicity for malaria; and a western African village exposed to a very intense transmission of P. falciparum. Antibodies directed to the two polypeptides were found at high titers in both populations. Furthermore, this response was observed in individuals lacking antibodies to the highly repetitive central sequence of the CS protein (NANP). The epitopes responsible for this recognition were mapped to the region 81-125 and 316-346 of the N- and C-termini, respectively. When the two populations were compared, both showed high titers of antibodies to the two flanking peptides. However, while 95% of the sera from African adults showed antibodies against the repeat region of the CS protein, only 37% of the Colombian adults studied had these antibodies. Furthermore, African donors of various ages exhibited different patterns of recognition of the two polypeptides. In African children less than five years of age, antibodies were found in comparable levels to Colombian adults; however, in older African donors, the response to NANP became dominant. These findings may reflect the skewing effect of the humoral response towards the central repetitive epitope under conditions of frequent exposure to malaria infections. The production of such polypeptides encompassing regions that contain multiple epitopes for antibodies, T helper, and cytotoxic T lymphocyte epitopes would be advantageous in the generation of new and more efficient malaria vaccines.

摘要

在本研究中,我们分析了南美洲和非洲疟疾流行地区的供者血清对恶性疟原虫环子孢子(CS)蛋白氨基末端(氨基酸22 - 125)和羧基末端(289 - 390)区域合成多肽的识别情况。研究了两个群体:一个是哥伦比亚太平洋沿岸地区,疟疾流行程度较低;另一个是西非的一个村庄,该地区恶性疟原虫传播非常强烈。在这两个群体中均发现针对这两种多肽的抗体效价很高。此外,在缺乏针对CS蛋白高度重复中心序列(NANP)抗体的个体中也观察到了这种反应。负责这种识别的表位分别定位到N末端和C末端的81 - 125区域和316 - 346区域。当比较这两个群体时,两者对两种侧翼肽的抗体效价都很高。然而,虽然95%的非洲成年人血清显示出针对CS蛋白重复区域的抗体,但所研究的哥伦比亚成年人中只有37%有这些抗体。此外,不同年龄的非洲供者对这两种多肽的识别模式不同。在五岁以下的非洲儿童中,抗体水平与哥伦比亚成年人相当;然而,在年龄较大的非洲供者中,对NANP的反应占主导地位。这些发现可能反映了在频繁接触疟疾感染的情况下,体液免疫反应向中心重复表位的倾斜效应。生产包含针对抗体、辅助性T细胞和细胞毒性T淋巴细胞表位的多个表位区域的此类多肽,将有利于开发新的、更有效的疟疾疫苗。

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